1型葡萄糖转运体缺乏综合征临床和生化表型的儿科患者研究

Study of paediatric patients with the clinical and biochemical phenotype of glucose transporter type 1 deficiency syndrome.

作者信息

Jiménez Legido M, Cortés Ledesma C, Bernardino Cuesta B, López Marín L, Cantarín Extremera V, Pérez-Cerdá C, Pérez González B, López Martín E, González Gutiérrez-Solana L

机构信息

Sección de Neuropediatría, Hospital Infantil Universitario Niño Jesús, Madrid, España.

出版信息

Neurologia (Engl Ed). 2022 Mar;37(2):91-100. doi: 10.1016/j.nrl.2018.10.006. Epub 2019 Apr 29.

DOI:10.1016/j.nrl.2018.10.006

PMID:31047728

Abstract

INTRODUCTION

Glucose transporter type 1 (GLUT1) deficiency syndrome may present a range of phenotypes, including epilepsy, intellectual disability, and movement disorders. The majority of patients present low CSF glucose levels and/or defects in the SLC2A1 gene; however, some patients do not present low CSF glucose or SLC2A1 mutations, and may have other mutations in other genes with compatible phenotypes.

AIMS

We describe the clinical, biochemical, and genetic characteristics of the disease and perform a univariate analysis of a group of patients with clinical and biochemical phenotype of GLUT1 deficiency syndrome, with or without SLC2A1 mutations.

MATERIAL AND METHODS

The study included 13 patients meeting clinical and biochemical criteria for GLUT1 deficiency syndrome. SLC2A1 sequencing and multiplex ligation-dependent probe amplification were performed; exome sequencing was performed for patients with negative results.

RESULTS

Six patients presented the classic phenotype; 2 paroxysmal dyskinesia, 2 complex movement disorders, 2 early-onset absence seizures, and one presented drug-resistant childhood absence epilepsy. Six patients were positive for SLC2A1 mutations; in the other 5, another genetic defect was identified. No significant differences were observed between the 2 groups for age of onset, clinical presentation, microcephaly, intellectual disability, or response to ketogenic diet. Patients with SLC2A1 mutations presented more clinical changes in relation to diet (66.7% vs. 28.6% in the SLC2A1-negative group) and greater persistence of motor symptoms (66% vs. 28.6%); these differences were not statistically significant. Significant differences were observed for CSF glucose level (34.5 vs. 46mg/dL, P=.04) and CSF/serum glucose ratio (0.4 vs. 0.48, P<.05).

CONCLUSIONS

GLUT1 deficiency syndrome may be caused by mutations to genes other than SLC2A1 in patients with compatible phenotype, low CSF glucose level, and good response to the ketogenic diet.

摘要

引言

1型葡萄糖转运体（GLUT1）缺乏综合征可能呈现一系列表型，包括癫痫、智力残疾和运动障碍。大多数患者脑脊液葡萄糖水平低和/或SLC2A1基因存在缺陷；然而，一些患者脑脊液葡萄糖水平不低或无SLC2A1突变，可能在其他具有相似表型的基因中存在其他突变。

目的

我们描述该疾病的临床、生化和遗传特征，并对一组具有GLUT1缺乏综合征临床和生化表型的患者进行单因素分析，无论其是否存在SLC2A1突变。

材料与方法

该研究纳入了13例符合GLUT1缺乏综合征临床和生化标准的患者。进行了SLC2A1测序和多重连接依赖探针扩增；对结果为阴性的患者进行了外显子组测序。

结果

6例患者呈现经典表型；2例为发作性运动障碍，2例为复杂运动障碍，2例为早发性失神发作，1例为儿童耐药性失神癫痫。6例患者SLC2A1突变呈阳性；在另外5例中，鉴定出了另一种基因缺陷。两组在发病年龄、临床表现、小头畸形、智力残疾或生酮饮食反应方面未观察到显著差异。SLC2A1突变患者在饮食方面出现更多临床变化（SLC2A1阴性组为66.7% vs. 28.6%），运动症状持续时间更长（66% vs. 28.6%）；这些差异无统计学意义。在脑脊液葡萄糖水平（34.5 vs. 46mg/dL，P = 0.04）和脑脊液/血清葡萄糖比值（0.4 vs. 0.48，P < 0.05）方面观察到显著差异。